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151. Scatterometer wind services in Europe

Author

Stoffelen, Ad, Belmonte, Maria, Verhoef, Anton, Verspeek, Jeroen, Vogelzang, J., Portabella, Marcos, and Bentamy, Abderrahim

Abstract

2009 NASA Ocean Vector Wind Science Team Meeting, 18-20 May 2009 Boulder, CO

Published
2009

152. ASCAT Scatterometer wind data processing

Author

Portabella, Marcos, Stoffelen, Ad, Belmonte, Maria, Verhoef, Anton, Verspeek, Jeroen, and Vogelzang, J.

Subjects
Microwave remote sensing, Spatial filtering, ASCAT, education, Enginyeria electrònica [Àrees temàtiques de la UPC], ASCAT Scatterometer, Quality control, Sea surface winds, Non-linear Inversion, Quality Cintrol
Abstract

Martech 2009 Third Marine Technology Workshop, 19-20 november 2009, Vilanova i la Geltrú, Barcelona.-- 1 page

Published
2009

153. Analysis of the ASCAT wind inversion residual: towards an improved C-band geophysical model function

Author

Portabella, Marcos, Stoffelen, Ad, Belmonte, Maria, Verhoef, Anton, Verspeek, Jeroen, and Vogelzang, J.

Abstract

2008 NASA Ocean Vector Wind Science Team Meeting, 19-21 November 2008, Seattle, WA, The Advanced Scatterometer (ASCAT) instrument, a real aperture vertically polarised C-band radar with high radiometric stability, was launched onboard EUMETSAT’s MetOp in October 2006. Within the EUMETSAT Satellite Application Facilities (SAF), the Royal Netherlands Meteorological Institute (KNMI) has the responsibility of the ASCAT level 2 wind production. During the successful calibration and validation phase, in which the instrument has been precisely calibrated and outperforming in terms of retrieved wind accuracy, several aspects of the level 2 processing were reviewed, notably the forward modeling, the Quality Control (QC) and the wind retrieval. Several authors have shown that a proper characterization of the scatterometer inversion residual or Maximum Likelihood Estimator (MLE) is very useful for improving level 2 processing. Following previous experience with the European ERS scatterometer, we normalize the ASCAT MLE and look into its properties as a QC indicator and wind retrieval parameter. Furthermore, we show that by looking at the normalized MLE magnitude and sign, one can identify certain deficiencies in the Geophysical Model Function (GMF). This analysis sets the grounds for an improved C-band GMF, i.e., CMOD6

Published
2008

154. Quality of high resolution ASCAT wind fields

Author

Vogelzang, J., Stoffelen, Ad, Belmonte, Maria, Portabella, Marcos, Verhoef, Anton, and Verspeek, Jeroen

Abstract

EUMETSAT Meteorological Satellite Conference, 8-12 September 2008, Darmstadt, Germany.-- 7 pages, 6 figures, The Advanced Scatterometer (ASCAT) delivers high resolution measurements of the ocean surface vector winds since 2006. Level 2 processing is done with the ASCAT Wind Data Processor (AWDP). AWDP builds upon the experience gained with the European scatterometers on board ERS-1 and ERS-2 as well as the American SeaWinds scatterometer carried by QuikSCAT. It has several advanced features, in particular the Multiple Solution Scheme (MSS) and Two Dimensional Variational Ambiguity Removal (2DVAR). The effect of these features on the quality of the 25 km and 12.5 km ASCAT wind products is studied in this paper

Published
2008

155. The SeaWinds data processor

Author

Vogelzang, J., Stoffelen, Ad, Belmonte, Maria, Portabella, Marcos, Verhoef, Anton, and Verspeek, Jeroen

Abstract

EUMETSAT Meteorological Satellite Conference, 8-12 September 2008, Darmstadt, Germany.-- 6 pages, 5 figures, 1 table, SeaWinds on board QuikSCAT is a rotating beam Ku-band scatterometer, operational since 1999. The SeaWinds Data Processor (SDP) reprocesses the level 2 BUFR product. SDP has a number of advanced features, in particular the Multiple Solution Scheme (MSS) and Two Dimensional Variational Ambiguity Removal (2DVAR). The current operational version, SDP 1.5, is reviewed in this paper. It is shown that 2DVAR in combination with MSS is effective in removing observational noise in the SeaWinds observations in the nadir part of the swath. Before the end of 2008 version 2.0 of SDP will be released. It includes processing of the outer swath and improved variational quality control. In this paper some examples of SDP wind products will be shown and their quality will be assessed

Published
2008

156. EUMETSAT SAF wind services

Author

Stoffelen, Ad, Portabella, Marcos, Verhoef, Anton, Verspeek, Jeroen, Vogelzang, J., and Belmonte, Maria

Subjects
ComputerSystemsOrganization_COMPUTERSYSTEMIMPLEMENTATION, GeneralLiterature_INTRODUCTORYANDSURVEY, ComputerApplications_COMPUTERSINOTHERSYSTEMS, GeneralLiterature_MISCELLANEOUS
Abstract

NASA Ocean Vector Winds Science Team Workshop, 19-21 November 2008, Seattle, USA

Published
2008

158. Measuring naturally acquired ex vivo IFN-γ responses to Plasmodium falciparum cell-traversal protein for ookinetes and sporozoites (CelTOS) in Ghanaian adults

Author

Anum, Dorothy, primary, Kusi, Kwadwo A, additional, Ganeshan, Harini, additional, Hollingdale, Michael R, additional, Ofori, Michael F, additional, Koram, Kwadwo A, additional, Gyan, Ben A, additional, Adu-Amankwah, Susan, additional, Badji, Edem, additional, Huang, Jun, additional, Belmonte, Maria, additional, Banania, Glenna J, additional, Kwofie, Theophilus B, additional, Villasante, Eileen, additional, Dodoo, Daniel, additional, and Sedegah, Martha, additional

Published
2015
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159. Sterile Immunity to Malaria after DNA Prime/Adenovirus Boost Immunization Is Associated with Effector Memory CD8+T Cells Targeting AMA1 Class I Epitopes

Author

Sedegah, Martha, primary, Hollingdale, Michael R., additional, Farooq, Fouzia, additional, Ganeshan, Harini, additional, Belmonte, Maria, additional, Kim, Yohan, additional, Peters, Bjoern, additional, Sette, Alessandro, additional, Huang, Jun, additional, McGrath, Shannon, additional, Abot, Esteban, additional, Limbach, Keith, additional, Shi, Meng, additional, Soisson, Lorraine, additional, Diggs, Carter, additional, Chuang, Ilin, additional, Tamminga, Cindy, additional, Epstein, Judith E., additional, Villasante, Eileen, additional, and Richie, Thomas L., additional

Published
2014
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160. Vaxfectin (registered trademark) Enhances Both Antibody and In Vitro T Cell Responses to Each Component of a 5-gene Plasmodium falciparum Plasmid DNA Vaccine Mixture Administered at Low Doses

Author

NAVAL MEDICAL RESEARCH CENTER SILVER SPRING MD MALARIA PROGRAM, Sedegah, Martha, Rogers, William O, Belmonte, Maria, Belmonte, Arnel, Banania, Glenna, Patterson, Noelle B, Rusalov, Denis, Ferrari, Marilyn, Richie, Thomas L, Doolan, Denise L, NAVAL MEDICAL RESEARCH CENTER SILVER SPRING MD MALARIA PROGRAM, Sedegah, Martha, Rogers, William O, Belmonte, Maria, Belmonte, Arnel, Banania, Glenna, Patterson, Noelle B, Rusalov, Denis, Ferrari, Marilyn, Richie, Thomas L, and Doolan, Denise L

Abstract

We previously reported the capacity of the cationic lipid-based formulation, Vaxfectin (registered trademark) to enhance the immunogenicity and protective efficacy of a low dose plasmid DNA vaccine against Plasmodium yoelii malaria in mice. Here, we have extended this finding to human Plasmodium falciparum genes, evaluating the immune enhancing effect of Vaxfectin (registered trademark) formulation on a mixture designated CSLAM of five plasmid DNA vaccines encoding antigens from the sporozoite (PfCSP, PfSSP2/TRAP), intrahepatic (PfLSA1), and erythrocytic (PfAMA1, PfMSP1) life cycle stages of P. falciparum administered at 2, 10 or 50 microgram doses. Vaxfectin (registered trademark) formulation enhanced both antibody and cellular immune responses ro each component of the multi-antigen vaccine mixture, as assessed by ELISA, IFAT, and IFN-gamma ELlspot, respectively. There was no apparent antigenic competition, as indicated by comparison of responses induced in mice immunized with PfCSP vs. CSLAM. These data showing that Vaxfectin (registered trademark) can enhance the immunogenicty of plasmid DNA vaccines administered at low doses per body weight, and in combinations, has important clinical implications for the development of a vaccine against malaria, as well as against other public health threats., Published in Vaccine, v28 p3055-3065, 2010. Sponsored in part by USAMRMC.

Published
2010

161. Identification and Localization of Minimal MHC-restricted CD8+ T Cell Epitopes within the Plasmodium falciparum AMA1 Protein

Author

NAVAL MEDICAL RESEARCH CENTER SILVER SPRING MD, Sedegah, Martha, Kim, Yohan, Peters, Bjoern, McGrath, Shannon, Ganeshan, Harini, Lejano, Jennylynn, Abot, Esteban, Banania, Glenna, Belmonte, Maria, Sayo, Renato, NAVAL MEDICAL RESEARCH CENTER SILVER SPRING MD, Sedegah, Martha, Kim, Yohan, Peters, Bjoern, McGrath, Shannon, Ganeshan, Harini, Lejano, Jennylynn, Abot, Esteban, Banania, Glenna, Belmonte, Maria, and Sayo, Renato

Abstract

Background: Plasmodium falciparum apical membrane antigen-1 (AMA1) is a leading malaria vaccine candidate antigen that is expressed by sporozoite, liver and blood stage parasites. Since CD8+ T cell responses have been implicated in protection against pre-erythrocytic stage malaria, this study was designed to identify MHC class I-restricted epitopes within AMA1. Methods: A recombinant adenovirus serotype 5 vector expressing P. falciparum AMA1 was highly immunogenic when administered to healthy, malaria-naive adult volunteers as determined by IFN-g ELISpot responses to peptide pools containing overlapping 15-mer peptides spanning full-length AMA1. Computerized algorithms (NetMHC software) were used to predict minimal MHC-restricted 8-10-mer epitope sequences within AMA1 15-mer peptides active in ELISpot. A subset of epitopes was synthesized and tested for induction of CD8+ T cell IFN-g responses by ELISpot depletion and ICS assays. A 3-dimensional model combining Domains I + II of P. falciparum AMA1 and Domain III of P. vivax AMA1 was used to map these epitopes. Results: Fourteen 8-10-mer epitopes were predicted to bind to HLA supertypes A01 (3 epitopes), A02 (4 epitopes) B08 (2 epitopes) and B44 (5 epitopes). Nine of the 14 predicted epitopes were recognized in ELISpot or ELISpot and ICS assays by one or more volunteers. Depletion of T cell subsets confirmed that these epitopes were CD8+ T cell-dependent. A mixture of the 14 minimal epitopes was capable of recalling CD8+ T cell IFN-g responses from PBMC of immunized volunteers. Thirteen of the 14 predicted epitopes were polymorphic and the majority localized to the more conserved front surface of the AMA1 model structure. Conclusions: This study predicted 14 and confirmed nine MHC class I-restricted CD8+ T cell epitopes on AMA1 recognized in the context of seven HLA alleles. These HLA alleles belong to four HLA supertypes that have a phenotypic frequency between 23% - 100% in different human populations., Published in Malaria Journal, v9 n241 p1-16, 2010.

Published
2010

162. ASCAT Scatterometer wind data processing

Author

Portabella, Marcos, Stoffelen, Ad, Belmonte, Maria, Verhoef, Anton, Verspeek, Jeroen, Vogelzang, Jur, Portabella, Marcos, Stoffelen, Ad, Belmonte, Maria, Verhoef, Anton, Verspeek, Jeroen, and Vogelzang, Jur

Abstract

Peer Reviewed

Published
2010

163. High-resolution ASCAT scatterometer winds near the coast

Author

Portabella, Marcos, Stoffelen, Ad, Belmonte, Maria, Verhoef, Anton, Verspeek, Jeroen, Vogelzang, J., Portabella, Marcos, Stoffelen, Ad, Belmonte, Maria, Verhoef, Anton, Verspeek, Jeroen, and Vogelzang, J.

Abstract

The Advanced scatterometer, ASCAT, on MetOp-A was launched on 19 October 2006 as the third wind scatterometer currently in space joining up with the ERS-2 and the SeaWinds scatterometers. Scatterometers measure the radar backscatter from wind-generated cm-size gravity-capillary waves and provide high-resolution wind vector fields over the sea with high quality. In this paper we show progress in high resolution processing and its verification, and in processing closer to the coast

Published
2008

164. Ex vivo tetramer staining and cell surface phenotyping for early activation markers CD38 and HLA-DR to enumerate and characterize malaria antigen-specific CD8+ T-cells induced in human volunteers immunized with a Plasmodium falciparum adenovirus-vectored malaria vaccine expressing AMA1

Author

Schwenk, Robert, primary, Banania, Glenna, additional, Epstein, Judy, additional, Kim, Yohan, additional, Peters, Bjoern, additional, Belmonte, Maria, additional, Ganeshan, Harini, additional, Huang, Jun, additional, Reyes, Sharina, additional, Stryhn, Anette, additional, Ockenhouse, Christian F, additional, Buus, Soren, additional, Richie, Thomas L, additional, and Sedegah, Martha, additional

Published
2013
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165. Human adenovirus 5-vectoredPlasmodium falciparumNMRC-M3V-Ad-PfCA vaccine encoding CSP and AMA1 is safe, well-tolerated and immunogenic but does not protect against controlled human malaria infection

Author

Tamminga, Cindy, primary, Sedegah, Martha, additional, Maiolatesi, Santina, additional, Fedders, Charlotte, additional, Reyes, Sharina, additional, Reyes, Anatalio, additional, Vasquez, Carlos, additional, Alcorta, Yolanda, additional, Chuang, Ilin, additional, Spring, Michele, additional, Kavanaugh, Michael, additional, Ganeshan, Harini, additional, Huang, Jun, additional, Belmonte, Maria, additional, Abot, Esteban, additional, Belmonte, Arnel, additional, Banania, JoGlenna, additional, Farooq, Fouzia, additional, Murphy, Jittawadee, additional, Komisar, Jack, additional, Richie, Nancy O, additional, Bennett, Jason, additional, Limbach, Keith, additional, Patterson, Noelle B, additional, Bruder, Joseph T, additional, Shi, Meng, additional, Miller, Edward, additional, Dutta, Sheetij, additional, Diggs, Carter, additional, Soisson, Lorraine A, additional, Hollingdale, Michael R, additional, Epstein, Judith E, additional, and Richie, Thomas L, additional

Published
2013
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166. Identification of minimal human MHC-restricted CD8+ T-cell epitopes within the Plasmodium falciparum circumsporozoite protein (CSP)

Author

Sedegah, Martha, primary, Kim, Yohan, additional, Ganeshan, Harini, additional, Huang, Jun, additional, Belmonte, Maria, additional, Abot, Esteban, additional, Banania, Jo Glenna, additional, Farooq, Fouzia, additional, McGrath, Shannon, additional, Peters, Bjoern, additional, Sette, Alessandro, additional, Soisson, Lorraine, additional, Diggs, Carter, additional, Doolan, Denise L, additional, Tamminga, Cindy, additional, Villasante, Eileen, additional, Hollingdale, Michael R, additional, and Richie, Thomas L, additional

Published
2013
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167. DNA Prime/Adenovirus Boost Malaria Vaccine Encoding P. falciparum CSP and AMA1 Induces Sterile Protection Associated with Cell-Mediated Immunity

Author

Chuang, Ilin, primary, Sedegah, Martha, additional, Cicatelli, Susan, additional, Spring, Michele, additional, Polhemus, Mark, additional, Tamminga, Cindy, additional, Patterson, Noelle, additional, Guerrero, Melanie, additional, Bennett, Jason W., additional, McGrath, Shannon, additional, Ganeshan, Harini, additional, Belmonte, Maria, additional, Farooq, Fouzia, additional, Abot, Esteban, additional, Banania, Jo Glenna, additional, Huang, Jun, additional, Newcomer, Rhonda, additional, Rein, Lisa, additional, Litilit, Dianne, additional, Richie, Nancy O., additional, Wood, Chloe, additional, Murphy, Jittawadee, additional, Sauerwein, Robert, additional, Hermsen, Cornelus C., additional, McCoy, Andrea J., additional, Kamau, Edwin, additional, Cummings, James, additional, Komisar, Jack, additional, Sutamihardja, Awalludin, additional, Shi, Meng, additional, Epstein, Judith E., additional, Maiolatesi, Santina, additional, Tosh, Donna, additional, Limbach, Keith, additional, Angov, Evelina, additional, Bergmann-Leitner, Elke, additional, Bruder, Joseph T., additional, Doolan, Denise L., additional, King, C. Richter, additional, Carucci, Daniel, additional, Dutta, Sheetij, additional, Soisson, Lorraine, additional, Diggs, Carter, additional, Hollingdale, Michael R., additional, Ockenhouse, Christian F., additional, and Richie, Thomas L., additional

Published
2013
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171. Adenovirus 5-Vectored P. falciparum Vaccine Expressing CSP and AMA1. Part A: Safety and Immunogenicity in Seronegative Adults

Author

Sedegah, Martha, primary, Tamminga, Cindy, additional, McGrath, Shannon, additional, House, Brent, additional, Ganeshan, Harini, additional, Lejano, Jennylynn, additional, Abot, Esteban, additional, Banania, Glenna J., additional, Sayo, Renato, additional, Farooq, Fouzia, additional, Belmonte, Maria, additional, Manohar, Nalini, additional, Richie, Nancy O., additional, Wood, Chloe, additional, Long, Carole A., additional, Regis, David, additional, Williams, Francis T., additional, Shi, Meng, additional, Chuang, Ilin, additional, Spring, Michele, additional, Epstein, Judith E., additional, Mendoza-Silveiras, Jose, additional, Limbach, Keith, additional, Patterson, Noelle B., additional, Bruder, Joseph T., additional, Doolan, Denise L., additional, King, C. Richter, additional, Soisson, Lorraine, additional, Diggs, Carter, additional, Carucci, Daniel, additional, Dutta, Sheetij, additional, Hollingdale, Michael R., additional, Ockenhouse, Christian F., additional, and Richie, Thomas L., additional

Published
2011
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172. Adenovirus-5-Vectored P. falciparum Vaccine Expressing CSP and AMA1. Part B: Safety, Immunogenicity and Protective Efficacy of the CSP Component

Author

Tamminga, Cindy, primary, Sedegah, Martha, additional, Regis, David, additional, Chuang, Ilin, additional, Epstein, Judith E., additional, Spring, Michele, additional, Mendoza-Silveiras, Jose, additional, McGrath, Shannon, additional, Maiolatesi, Santina, additional, Reyes, Sharina, additional, Steinbeiss, Victoria, additional, Fedders, Charlotte, additional, Smith, Kathryn, additional, House, Brent, additional, Ganeshan, Harini, additional, Lejano, Jennylynn, additional, Abot, Esteban, additional, Banania, Glenna J., additional, Sayo, Renato, additional, Farooq, Fouzia, additional, Belmonte, Maria, additional, Murphy, Jittawadee, additional, Komisar, Jack, additional, Williams, Jackie, additional, Shi, Meng, additional, Brambilla, Donald, additional, Manohar, Nalini, additional, Richie, Nancy O., additional, Wood, Chloe, additional, Limbach, Keith, additional, Patterson, Noelle B., additional, Bruder, Joseph T., additional, Doolan, Denise L., additional, King, C. Richter, additional, Diggs, Carter, additional, Soisson, Lorraine, additional, Carucci, Daniel, additional, Levine, Gail, additional, Dutta, Sheetij, additional, Hollingdale, Michael R., additional, Ockenhouse, Christian F., additional, and Richie, Thomas L., additional

Published
2011
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173. Vaxfectin® enhances both antibody and in vitro T cell responses to each component of a 5-gene Plasmodium falciparum plasmid DNA vaccine mixture administered at low doses

Author

Sedegah, Martha, primary, Rogers, William O., additional, Belmonte, Maria, additional, Belmonte, Arnel, additional, Banania, Glenna, additional, Patterson, Noelle B., additional, Rusalov, Denis, additional, Ferrari, Marilyn, additional, Richie, Thomas L., additional, and Doolan, Denise L., additional

Published
2010
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178. Successful Induction of CD8 T Cell-Dependent Protection Against Malaria by Sequential Immunization with DNA and Recombinant Poxvirus of Neonatal Mice Born to Immune Mothers

Author

Sedegah, Martha, primary, Belmonte, Maria, additional, Epstein, Judith E., additional, Siegrist, Claire-Anne, additional, Weiss, Walter R., additional, Jones, Trevor R., additional, Lu, Minh, additional, Carucci, Daniel J., additional, and Hoffman, Stephen L., additional

Published
2003
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179. Persistence of Protective Immunity to Malaria Induced by DNA Priming and Poxvirus Boosting: Characterization of Effector and Memory CD8+-T-Cell Populations

Author

Sedegah, Martha, primary, Brice, Gary T., additional, Rogers, William O., additional, Doolan, Denise L., additional, Charoenvit, Yupin, additional, Jones, Trevor R., additional, Majam, Victoria F., additional, Belmonte, Arnel, additional, Lu, Minh, additional, Belmonte, Maria, additional, Carucci, Daniel J., additional, and Hoffman, Stephen L., additional

Published
2002
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180. Tendencia en la vacunación en personas con infección por VIH participantes en la Encuesta Hospitalaria de pacientes con VIH, 2006-2021

Author

Hernando, Victoria, Suárez, Lucia, Gutiérrez, Gonzalo, López, Juan Carlos, Navarro-Soler, Roser, Cabello, Alfonso, Sanz, Jesús, Suarez-García, Inés, Fernández, Maria Teresa, Losa, Juan Emilio, Pérez, Jose Luis, Ramos-Ruperto, Luis, Pérez-Elías, Maria Jesús, Aayuni, Wafa Ben Cheikh El, Cuesta, Mar, González, Gustavo, Izquierdo, Ana, Viloria, Luis, López, Irene, Martínez, Eva, Castrillejo, Daniel, Jaume Amengual, Maria Glòria, Belmonte, Maria Antonia, Arraiza, Antonio, de la Torre, Javier, Miqueleiz, Estrella, Marcos, Henar, Ruiz-Algueró, Marta, Villegas, Teresa, Simón, Lorena, and Diaz, Asuncion

Abstract

Evaluar la tendencia en la vacunación de hepatitis A, hepatitis B, neumococo, tétanos y gripe estacional en personas con infección por VIH, y analizar sus factores asociados.

Published
2023
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181. Ex vivo tetramer staining and cell surface phenotyping for early activation markers CD38 and HLA-DR to enumerate and characterize malaria antigen-specific CD8+ T-cells induced in human volunteers immunized with a Plasmodium falciparum adenovirus-vectored malaria vaccine expressing AMA1

Author

Schwenk, Robert, Banania, Glenna, Epstein, Judy, Yohan Kim, Peters, Bjoern, Belmonte, Maria, Ganeshan, Harini, Jun Huang, Reyes, Sharina, Stryhn, Anette, Ockenhouse, Christian F., Buus, Soren, Richie, Thomas L., and Sedegah, Martha

Subjects
MALARIA diagnosis, CD81 antigen, HLA-DR antigens, T cell receptors, TETRAMERS (Oligomers), PROTEIN analysis
Abstract

Background Malaria is responsible for up to a 600,000 deaths per year; conveying an urgent need for the development of a malaria vaccine. Studies with whole sporozoite vaccines in mice and nonhuman primates have shown that sporozoite-induced CD8+ T cells targeting liver stage antigens can mediate sterile protection. There is a need for a direct method to identify and phenotype malaria vaccine-induced CD8+ T cells in humans. Methods Fluorochrome-labelled tetramers consisting of appropriate MHC class I molecules in complex with predicted binding peptides derived from Plasmodium falciparum AMA-1 were used to label ex vivo AMA-1 epitope specific CD8+ T cells from research subjects responding strongly to immunization with the NMRC-M3V-Ad-PfCA (adenovirus-vectored) malaria vaccine. The identification of these CD8+ T cells on the basis of their expression of early activation markers was also investigated. Results Analyses by flow cytometry demonstrated that two of the six tetramers tested: TLDEMRHFY: HLA-A"01:01 and NEVVVKEEY: HLA-B"18:01, labelled tetramerspecific CD8+ T cells from two HLA-A"01:01 volunteers and one HLA-B"18:01 volunteer, respectively. By contrast, post-immune CD8+ T cells from all six of the immunized volunteers exhibited enhanced expression of the CD38 and HLA-DRhi early activation markers. For the three volunteers with positive tetramer staining, the early activation phenotype positive cells included essentially all of the tetramer positive, malaria epitopespecific CD8+ T cells suggesting that the early activation phenotype could identify all malaria vaccine-induced CD8+ T cells without prior knowledge of their exact epitope specificity Conclusions The results demonstrated that class I tetramers can identify ex vivo malaria vaccine antigenspecific CD8+ T cells and could therefore be used to determine their frequency, cell surface phenotype and transcription factor usage. The results also demonstrated that vaccine antigenspecific CD8+ T cells could be identified by activation markers without prior knowledge of their antigen-specificity, using a subunit vaccine for proof-of-concept. Whether, whole parasite or adjuvanted protein vaccines will also induce {CD38 and HLA-DRhi}+ CD8+ T cells populations reflective of the antigen-specific response will the subject of future investigations. [ABSTRACT FROM AUTHOR]

Published
2013
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182. DNA Prime/Adenovirus Boost Malaria Vaccine Encoding P. falciparum CSP and AMA1 Induces Sterile Protection Associated with Cell-Mediated Immunity.

Author

Chuang, Ilin, Sedegah, Martha, Cicatelli, Susan, Spring, Michele, Polhemus, Mark, Tamminga, Cindy, Patterson, Noelle, Guerrero, Melanie, Bennett, Jason W., McGrath, Shannon, Ganeshan, Harini, Belmonte, Maria, Farooq, Fouzia, Abot, Esteban, Banania, Jo Glenna, Huang, Jun, Newcomer, Rhonda, Rein, Lisa, Litilit, Dianne, and Richie, Nancy O.

Subjects
ADENOVIRUSES, MALARIA vaccines, CIRCUMSPOROZOITE protein, APICAL membrane antigen 1, CELLULAR immunity, MALARIA prevention, ANTIBODY formation, SEROPREVALENCE
Abstract

Background: Gene-based vaccination using prime/boost regimens protects animals and humans against malaria, inducing cell-mediated responses that in animal models target liver stage malaria parasites. We tested a DNA prime/adenovirus boost malaria vaccine in a Phase 1 clinical trial with controlled human malaria infection. Methodology/Principal Findings: The vaccine regimen was three monthly doses of two DNA plasmids (DNA) followed four months later by a single boost with two non-replicating human serotype 5 adenovirus vectors (Ad). The constructs encoded genes expressing P. falciparum circumsporozoite protein (CSP) and apical membrane antigen-1 (AMA1). The regimen was safe and well-tolerated, with mostly mild adverse events that occurred at the site of injection. Only one AE (diarrhea), possibly related to immunization, was severe (Grade 3), preventing daily activities. Four weeks after the Ad boost, 15 study subjects were challenged with P. falciparum sporozoites by mosquito bite, and four (27%) were sterilely protected. Antibody responses by ELISA rose after Ad boost but were low (CSP geometric mean titer 210, range 44–817; AMA1 geometric mean micrograms/milliliter 11.9, range 1.5–102) and were not associated with protection. Ex vivo IFN-γ ELISpot responses after Ad boost were modest (CSP geometric mean spot forming cells/million peripheral blood mononuclear cells 86, range 13–408; AMA1 348, range 88–1270) and were highest in three protected subjects. ELISpot responses to AMA1 were significantly associated with protection (p = 0.019). Flow cytometry identified predominant IFN-γ mono-secreting CD8+ T cell responses in three protected subjects. No subjects with high pre-existing anti-Ad5 neutralizing antibodies were protected but the association was not statistically significant. Significance: The DNA/Ad regimen provided the highest sterile immunity achieved against malaria following immunization with a gene-based subunit vaccine (27%). Protection was associated with cell-mediated immunity to AMA1, with CSP probably contributing. Substituting a low seroprevalence vector for Ad5 and supplementing CSP/AMA1 with additional antigens may improve protection. Trial Registration: ClinicalTrials.govNCT00870987. [ABSTRACT FROM AUTHOR]

Published
2013
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183. Identification and localization of minimalMHC-restricted CD8+ T cell epitopes withinthe Plasmodium falciparum AMA1 protein.

Author

Sedegah, Martha, Yohan Kim, Peters, Bjoern, McGrath, Shannon, Ganeshan, Harini, Lejano, Jennylynn, Abot, Esteban, Banania, Glenna, Belmonte, Maria, Sayo, Renato, Farooq, Fouzia, Doolan, Denise L., Regis, David, Tamminga, Cindy, Ilin Chuang, Bruder, Joseph T., King, C. Richter, Ockenhouse, Christian F., Faber, Bart, and Remarque, Edmond

Subjects
PLASMODIUM falciparum, MALARIA, EPITOPES, HLA histocompatibility antigens, PREVENTIVE medicine
Abstract

Background: Plasmodium falciparum apical membrane antigen-1 (AMA1) is a leading malaria vaccine candidate antigen that is expressed by sporozoite, liver and blood stage parasites. Since CD8+ T cell responses have been implicated in protection against pre-erythrocytic stage malaria, this study was designed to identify MHC class I-restricted epitopes within AMA1. Methods: A recombinant adenovirus serotype 5 vector expressing P. falciparum AMA1 was highly immunogenic when administered to healthy, malaria-naive adult volunteers as determined by IFN-γ ELISpot responses to peptide pools containing overlapping 15-mer peptides spanning full-length AMA1. Computerized algorithms (NetMHC software) were used to predict minimal MHC-restricted 8-10-mer epitope sequences within AMA1 15-mer peptides active in ELISpot. A subset of epitopes was synthesized and tested for induction of CD8+ T cell IFN-γ responses by ELISpot depletion and ICS assays. A 3-dimensional model combining Domains I + II of P. falciparum AMA1 and Domain III of P. vivax AMA1 was used to map these epitopes. Results: Fourteen 8-10-mer epitopes were predicted to bind to HLA supertypes A01 (3 epitopes), A02 (4 epitopes), B08 (2 epitopes) and B44 (5 epitopes). Nine of the 14 predicted epitopes were recognized in ELISpot or ELISpot and ICS assays by one or more volunteers. Depletion of T cell subsets confirmed that these epitopes were CD8+ T cell-dependent. A mixture of the 14 minimal epitopes was capable of recalling CD8+ T cell IFN-γ responses from PBMC of immunized volunteers. Thirteen of the 14 predicted epitopes were polymorphic and the majority localized to the more conserved front surface of the AMA1 model structure. Conclusions: This study predicted 14 and confirmed nine MHC class I-restricted CD8+ T cell epitopes on AMA1 recognized in the context of seven HLA alleles. These HLA alleles belong to four HLA supertypes that have a phenotypic frequency between 23% - 100% in different human populations. [ABSTRACT FROM AUTHOR]

Published
2010
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184. Hepatic steatosis, carotid atherosclerosis and metab olic syndrome: the STEATO Study.

Author

Carallo, Claudio, Mancuso, Gerardo, Mauro, Gaetano, Laghi, Ferdinando, Madafferi, Bruno, Irace, Concetta, Gnasso, Agostino, Scavelli, Faustina, Dell’Aquila, Ferruccio, Bartone, Mosè, Gullo, Francesco, Ferraro, Maria, Spagnuolo, Vitaliano, Belmonte, Maria, Ferrara, Antonio, Rotondaro, Antonio, Brandolino, Nicola, Parasporo, Francesca, and Scopelliti, Francesco

Subjects
LIVER diseases, ATHEROSCLEROSIS, METABOLIC syndrome, FATTY degeneration, TYPE 2 diabetes, AMINOTRANSFERASES, CARDIOVASCULAR diseases
Abstract

Hepatic steatosis is frequently observed in subjects with metabolic syndrome (MS). In type 2 diabetics, it is independently associated with cardiovascular diseases. In order to confirm and extend this finding, a large group of patients with risk factors for atherosclerosis was studied. Carotid atherosclerosis was investigated by echo-Doppler, and hepatic steatosis by ultrasound and transaminase values. Strict exclusion criteria were chosen in order to avoid secondary forms of fatty liver and interference on transaminase values. Among 970 enrolled patients, about 20% were diabetics, half had MS and 76% presented echographic hepatic steatosis. In multivariate analyses, fatty liver and MS were associated with carotid atherosclerosis [odds ratio (95% confidence intervals) 2.15 (1.27–3.63) and 1.72 (1.12–2.64), respectively], whereas HOMA index was not. Aspartate aminotransferase and alanine aminotransferase were not independently associated with carotid atherosclerosis, whereas gamma-glutamyl transferase showed a link with atherosclerosis beyond MS and steatosis presence. The analyses of the 780 non diabetics recruited showed similar results. The results of the present study demonstrate that hepatic steatosis measured by echography is associated with carotid atherosclerosis in a large population mostly carrying cardiovascular or metabolic risk factors, independently of MS, cardiovascular diseases, diabetes mellitus and/or insulin resistance. [ABSTRACT FROM AUTHOR]

Published
2009
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185. Human adenovirus 5-vectored Plasmodium falciparumNMRC-M3V-Ad-PfCA vaccine encoding CSP and AMA1 is safe, well-tolerated and immunogenic but does not protect against controlled human malaria infection

Author

Tamminga, Cindy, Sedegah, Martha, Maiolatesi, Santina, Fedders, Charlotte, Reyes, Sharina, Reyes, Anatalio, Vasquez, Carlos, Alcorta, Yolanda, Chuang, Ilin, Spring, Michele, Kavanaugh, Michael, Ganeshan, Harini, Huang, Jun, Belmonte, Maria, Abot, Esteban, Belmonte, Arnel, Banania, JoGlenna, Farooq, Fouzia, Murphy, Jittawadee, Komisar, Jack, Richie, Nancy O, Bennett, Jason, Limbach, Keith, Patterson, Noelle B, Bruder, Joseph T, Shi, Meng, Miller, Edward, Dutta, Sheetij, Diggs, Carter, Soisson, Lorraine A, Hollingdale, Michael R, Epstein, Judith E, and Richie, Thomas L

Abstract

Background: In a prior study, a DNA prime / adenovirus boost vaccine (DNA/Ad) expressing P. falciparumcircumsporozoite protein (CSP) and apical membrane antigen-1 (AMA1) (NMRC-M3V-D/Ad-PfCA Vaccine) induced 27% protection against controlled human malaria infection (CHMI). To investigate the contribution of DNA priming, we tested the efficacy of adenovirus vaccine alone (NMRC-M3V-Ad-PfCA ) in a Phase 1 clinical trial.Methodology/Principal Findings: The regimen was a single intramuscular injection with two non-replicating human serotype 5 adenovectors encoding CSP and AMA1, respectively. One x 1010particle units of each construct were combined prior to administration. The regimen was safe and well-tolerated. Four weeks later, 18 study subjects received P. falciparumCHMI administered by mosquito bite. None were fully protected although one showed delayed onset of parasitemia. Antibody responses were low, with geometric mean CSP ELISA titer of 381 (range < 50–1626) and AMA1 ELISA of 4.95 µg/mL (range 0.2–38). Summed ex vivo IFN-γ ELISpot responses to overlapping peptides were robust, with geometric mean spot forming cells/million peripheral blood mononuclear cells [sfc/m] for CSP of 273 (range 38–2550) and for AMA1 of 1303 (range 435–4594). CD4+ and CD8+ T cell IFN-γ responses to CSP were positive by flow cytometry in 25% and 56% of the research subjects, respectively, and to AMA1 in 94% and 100%, respectively.Significance: In contrast to DNA/Ad, Ad alone did not protect against CHMI despite inducing broad, cell-mediated immunity, indicating that DNA priming is required for protection by the adenovirus-vectored vaccine. ClinicalTrials.gov Identifier: NCT00392015.

Published
2013
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186. Ablative Radiation Therapy for Unfavorable Prostate Tumors (ABRUPT): Preliminary Analysis of Toxicity and Quality of Life from a Prospective Study.

Author

Arcangeli, Stefano, Chissotti, Chiara, Ferrario, Federica, Lucchini, Raffaella, Belmonte, Maria, Purrello, Giorgio, Colciago, Riccardo Ray, De Ponti, Elena, Faccenda, Valeria, and Panizza, Denis

Subjects
*ANDROGEN deprivation therapy, *LOGISTIC regression analysis, *STANDARD deviations, *MULTIVARIATE analysis, *PROSTATE tumors
Abstract

To assess late gastrointestinal (GI) and genitourinary (GU) side effects in patients with organ-confined unfavorable prostate cancer (PCa) treated with single-dose ablative radiation therapy (SDRT). Thirty patients enrolled in a single-arm prospective trial received 24 Gy SDRT to the whole prostate with urethra-sparing and organ motion control delivered on a Linac platform with a 10 MV flattening filter-free single partial arc. Androgen deprivation therapy was prescribed as per standard of care. Treatment-related acute and late GU and GI toxicities (Common Terminology Criteria for Adverse Events_v5 scale) and quality of life (QoL) outcomes (European Organisation for Research and Treatment of Cancer [EORTC] QLQ-PR25/C30, International Prostate Symptom Score [IPSS]) were assessed at different time points. Minimal important difference (MID) was established as a change of >0.5 pooled standard deviations from baseline. Statistical analysis included analysis of variance and logistic regression. Median follow-up was 18 months (range, 6-31 months), with no ≥G3 late side effects observed. G2 late GI and G2 late GU toxicities occurred in 1 and 2 patients, respectively. GI toxicity of any grade correlated with maximum rectal dose (P =.021). Lower baseline QoL score (P =.025), higher baseline IPSS score (P =.049), acute GU toxicity (P =.029), and acute urinary domain MID (P =.045) predicted GU toxicity of any grade. In multivariate analysis (MVA), only baseline QoL score (odds ratio [OR], 0.95, P =.031) and acute GU toxicity (OR, 8.4, P =.041) remained significant. Significant QoL change was observed only in the urinary domain (P =.005), with a median increase from 8 to 17. Late urinary MID correlated with acute urinary MID (P =.003), acute QoL MID (P =.029), acute GU toxicity (P =.030), and lower baseline urinary score (P =.033). In MVA, only acute urinary MID predicted late urinary MID (OR, 9.7, P =.035). Our findings provide promising data on the feasibility and safety of 24 Gy whole-gland SDRT with urethra-sparing and organ motion control, in association with androgen deprivation therapy and an adequate prophylactic medication, in organ-confined unfavorable PCa. Long-term follow-up is needed to confirm these results. [ABSTRACT FROM AUTHOR]

Published
2024
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187. MOESM1 of Measurement of ex vivo ELISpot interferon-gamma recall responses to Plasmodium falciparum AMA1 and CSP in Ghanaian adults with natural exposure to malaria

Author

Harini Ganeshan, Kwadwo Kusi, Anum, Dorothy, Hollingdale, Michael, Bjoern Peters, Yohan Kim, Tetteh, John, Ofori, Michael, Gyan, Ben, Kwadwo Koram, Huang, Jun, Belmonte, Maria, Banania, Jo, Dodoo, Daniel, Villasante, Eileen, and Sedegah, Martha

Subjects
TheoryofComputation_COMPUTATIONBYABSTRACTDEVICES, ComputingMethodologies_PATTERNRECOGNITION, animal structures, fungi, parasitic diseases, complex mixtures, 3. Good health
Abstract

Additional file 1: Table S1. Peptide composition of the CSP 15mer peptide pools.

188. MOESM1 of Measurement of ex vivo ELISpot interferon-gamma recall responses to Plasmodium falciparum AMA1 and CSP in Ghanaian adults with natural exposure to malaria

Author

Harini Ganeshan, Kwadwo Kusi, Anum, Dorothy, Hollingdale, Michael, Bjoern Peters, Yohan Kim, Tetteh, John, Ofori, Michael, Gyan, Ben, Kwadwo Koram, Huang, Jun, Belmonte, Maria, Banania, Jo, Dodoo, Daniel, Villasante, Eileen, and Sedegah, Martha

Subjects
TheoryofComputation_COMPUTATIONBYABSTRACTDEVICES, ComputingMethodologies_PATTERNRECOGNITION, animal structures, fungi, parasitic diseases, complex mixtures, 3. Good health
Abstract

Additional file 1: Table S1. Peptide composition of the CSP 15mer peptide pools.

189. MOESM2 of Measurement of ex vivo ELISpot interferon-gamma recall responses to Plasmodium falciparum AMA1 and CSP in Ghanaian adults with natural exposure to malaria

Author

Harini Ganeshan, Kwadwo Kusi, Anum, Dorothy, Hollingdale, Michael, Bjoern Peters, Yohan Kim, Tetteh, John, Ofori, Michael, Gyan, Ben, Kwadwo Koram, Huang, Jun, Belmonte, Maria, Banania, Jo, Dodoo, Daniel, Villasante, Eileen, and Sedegah, Martha

Subjects
fungi, parasitic diseases, complex mixtures, 3. Good health
Abstract

Additional file 2: Table S2. Peptide composition of the AMA1 15mer peptide pools.

190. MOESM2 of Measurement of ex vivo ELISpot interferon-gamma recall responses to Plasmodium falciparum AMA1 and CSP in Ghanaian adults with natural exposure to malaria

Author

Harini Ganeshan, Kwadwo Kusi, Anum, Dorothy, Hollingdale, Michael, Bjoern Peters, Yohan Kim, Tetteh, John, Ofori, Michael, Gyan, Ben, Kwadwo Koram, Huang, Jun, Belmonte, Maria, Banania, Jo, Dodoo, Daniel, Villasante, Eileen, and Sedegah, Martha

Subjects
fungi, parasitic diseases, complex mixtures, 3. Good health
Abstract

Additional file 2: Table S2. Peptide composition of the AMA1 15mer peptide pools.

192. White dwarf pollution by hydrated planetary remnants: hydrogen and metals in WD J204713.76–125908.9.

Author

Hoskin, Matthew J, Toloza, Odette, Gänsicke, Boris T, Raddi, Roberto, Koester, Detlev, Pala, Anna F, Manser, Christopher J, Farihi, Jay, Belmonte, Maria Teresa, Hollands, Mark, Gentile Fusillo, Nicola, and Swan, Andrew

Subjects
*VERY large telescopes, *HYDROGEN content of metals, *PLANETESIMALS, *SOLAR radiation, *WHITE dwarf stars, *OPTICAL spectroscopy, *POLLUTION, *SIDEROPHILE elements
Abstract

WD J204713.76–125908.9 is a new addition to the small class of white dwarfs with helium-dominated photospheres that exhibit strong Balmer absorption lines and atmospheric metal pollution. The exceptional abundances of hydrogen observed in these stars may be the result of accretion of water-rich rocky bodies. We obtained far-ultraviolet and optical spectroscopy of WD J204713.76–125908.9 using the Cosmic Origin Spectrograph on-board the Hubble Space Telescope and X-shooter on the Very Large Telescope, and identify photospheric absorption lines of nine metals: C, O, Mg, Si, P, S, Ca, Fe, and Ni. The abundance ratios are consistent with the steady-state accretion of exo-planetesimal debris rich in the volatile elements carbon and oxygen, and the transitional element sulphur, by factors of 17, 2, and 4, respectively, compared to the bulk Earth. The parent body has a composition akin to Solar system carbonaceous chondrites, and the inferred minimum mass, 1.6 × 1020 g, is comparable to an asteroid 23 km in radius. We model the composition of the disrupted parent body, finding from our simulations a median water mass fraction of 8 per cent. [ABSTRACT FROM AUTHOR]

Published
2020
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193. IMRAS—A clinical trial of mosquito-bite immunization with live, radiation-attenuated P. falciparum sporozoites: Impact of immunization parameters on protective efficacy and generation of a repository of immunologic reagents.

Author

Hickey, Bradley, Teneza-Mora, Nimfa, Lumsden, Joanne, Reyes, Sharina, Sedegah, Martha, Garver, Lindsey, Hollingdale, Michael R., Banania, Jo Glenna, Ganeshan, Harini, Dowler, Megan, Reyes, Anatalio, Tamminga, Cindy, Singer, Alexandra, Simmons, Alicia, Belmonte, Maria, Belmonte, Arnel, Huang, Jun, Inoue, Sandra, Velasco, Rachel, and Abot, Steve

Subjects
*LEUKAPHERESIS, *SPOROZOITES, *IMMUNIZATION, *CLINICAL trials, *BLOOD plasma, *VACCINE effectiveness
Abstract

Background: Immunization with radiation-attenuated sporozoites (RAS) by mosquito bite provides >90% sterile protection against Plasmodium falciparum (Pf) malaria in humans. RAS invade hepatocytes but do not replicate. CD8+ T cells recognizing parasite-derived peptides on the surface of infected hepatocytes are likely the primary protective mechanism. We conducted a randomized clinical trial of RAS immunization to assess safety, to achieve 50% vaccine efficacy (VE) against controlled human malaria infection (CHMI), and to generate reagents from protected and non-protected subjects for future identification of protective immune mechanisms and antigens. Methods: Two cohorts (Cohort 1 and Cohort 2) of healthy, malaria-naïve, non-pregnant adults age 18–50 received five monthly immunizations with infected (true-immunized, n = 21) or non-infected (mock-immunized, n = 5) mosquito bites and underwent homologous CHMI at 3 weeks. Immunization parameters were selected for 50% protection based on prior clinical data. Leukapheresis was done to collect plasma and peripheral blood mononuclear cells. Results: Adverse event rates were similar in true- and mock-immunized subjects. Two true- and two mock-immunized subjects developed large local reactions likely caused by mosquito salivary gland antigens. In Cohort 1, 11 subjects received 810–1235 infected bites; 6/11 (55%) were protected against CHMI vs. 0/3 mock-immunized and 0/6 infectivity controls (VE 55%). In Cohort 2, 10 subjects received 839–1131 infected bites with a higher first dose and a reduced fifth dose; 9/10 (90%) were protected vs. 0/2 mock-immunized and 0/6 controls (VE 90%). Three/3 (100%) protected subjects administered three booster immunizations were protected against repeat CHMI vs. 0/6 controls (VE 100%). Cohort 2 uniquely showed a significant rise in IFN-γ responses after the third and fifth immunizations and higher antibody responses to CSP. Conclusions: PfRAS were generally safe and well tolerated. Cohort 2 had a higher first dose, reduced final dose, higher antibody responses to CSP and significant rise of IFN-γ responses after the third and fifth immunizations. Whether any of these factors contributed to increased protection in Cohort 2 requires further investigation. A cryobank of sera and cells from protected and non-protected individuals was generated for future immunological studies and antigen discovery. Trial registration: ClinicalTrials.gov NCT01994525. [ABSTRACT FROM AUTHOR]

Published
2020
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194. Vaxfectin™ enhances immunogenicity and protective efficacy of P. yoelii circumsporozoite DNA vaccines

Author

Sedegah, Martha, Rogers, William O., Belmonte, Arnel, Belmonte, Maria, Banania, Glenna, Patterson, Noelle, Ferrari, Marilyn, Kaslow, David C., Carucci, Daniel J., Richie, Thomas L., and Doolan, Denise L.

Subjects
*NUCLEIC acids, *DNA, *GENES, *HEREDITY
Abstract

Abstract: We evaluated the capacity of the cationic lipid based formulation, Vaxfectin™, to enhance the immunogenicity and protective efficacy of DNA-based vaccine regimens in the Plasmodium yoelii murine malaria model. We immunized Balb/c mice with varying doses (0.4–50μg) of plasmid DNA (pDNA) encoding the P. yoelii circumsporozoite protein (PyCSP), either in a homologous DNA/DNA regimen (D-D) or a heterologous prime-boost DNA-poxvirus regimen (D-V). At the lowest pDNA doses, Vaxfectin™ substantially enhanced IFA titers, ELISPOT frequencies, and protective efficacy. Clinical trials of pDNA vaccines have often used low pDNA doses based on a per kilogram weight basis. Formulation of pDNA vaccines in Vaxfectin™ may improve their potency in human clinical trials. [Copyright &y& Elsevier]

Published
2006
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195. D2.4 Data products validation report

Author

Oscar Rosario Belfiore, Salvatore Falanga Bolognesi and Alfonso Calera Belmonte, Maria Calera, Violeta Domnica Poenaru, Stelios Kotsopoulos, Elena Navarro, Luciano Mateos

Abstract

This document is an update of D2.3. and aims to describe the validation process of the data products provided by DIANA. For each DIANA data product –i) Crop classification, ii) Maps of irrigated area, iii) Crop evapotranspiration, iv) Net Irrigation requirements, v) Gross irrigation requirements, vi) Meteorological products - the validation and evaluation were performed. From the methodological point of view, data products listed in this document were defined considering “Users’ and stakeholders’ Requirements Analysis” and “Data requirements manual” described respectively in the deliverable D1.1 and D2.2. This approach ensures to meet the realities in which to apply DIANA services addressing the users’ requirements adequately regarding spatial, temporal and spectral resolution and by extending the operational capabilities of the platform offered.

Published
2020
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196. From Observation to Information and Users: The Copernicus Marine Service Perspective

Author

Pierre Yves Le Traon, Antonio Reppucci, Enrique Alvarez Fanjul, Lotfi Aouf, Arno Behrens, Maria Belmonte, Abderrahim Bentamy, Laurent Bertino, Vittorio Ernesto Brando, Matilde Brandt Kreiner, Mounir Benkiran, Thierry Carval, Stefania A. Ciliberti, Hervé Claustre, Emanuela Clementi, Giovanni Coppini, Gianpiero Cossarini, Marta De Alfonso Alonso-Muñoyerro, Anne Delamarche, Gerald Dibarboure, Frode Dinessen, Marie Drevillon, Yann Drillet, Yannice Faugere, Vicente Fernández, Andrew Fleming, M. Isabel Garcia-Hermosa, Marcos García Sotillo, Gilles Garric, Florent Gasparin, Cedric Giordan, Marion Gehlen, Marilaure L. Gregoire, Stephanie Guinehut, Mathieu Hamon, Chris Harris, Fabrice Hernandez, Jørgen B. Hinkler, Jacob Hoyer, Juha Karvonen, Susan Kay, Robert King, Thomas Lavergne, Benedicte Lemieux-Dudon, Leonardo Lima, Chongyuan Mao, Matthew J. Martin, Simona Masina, Angelique Melet, Bruno Buongiorno Nardelli, Glenn Nolan, Ananda Pascual, Jenny Pistoia, Atanas Palazov, Jean Francois Piolle, Marie Isabelle Pujol, Anne Christine Pequignet, Elisaveta Peneva, Begoña Pérez Gómez, Loic Petit de la Villeon, Nadia Pinardi, Andrea Pisano, Sylvie Pouliquen, Rebecca Reid, Elisabeth Remy, Rosalia Santoleri, John Siddorn, Jun She, Joanna Staneva, Ad Stoffelen, Marina Tonani, Luc Vandenbulcke, Karina von Schuckmann, Gianluca Volpe, Cecilie Wettre, Anna Zacharioudaki, Le Traon, Pierre Yve, Reppucci, Antonio, Alvarez Fanjul, Enrique, Aouf, Lotfi, Behrens, Arno, Belmonte, Maria, Bentamy, Abderrahim, Bertino, Laurent, Brando, Vittorio Ernesto, Kreiner, Matilde Brandt, Benkiran, Mounir, Carval, Thierry, Ciliberti, Stefania A., Claustre, Hervé, Clementi, Emanuela, Coppini, Giovanni, Cossarini, Gianpiero, De Alfonso Alonso-Muñoyerro, Marta, Delamarche, Anne, Dibarboure, Gerald, Dinessen, Frode, Drevillon, Marie, Drillet, Yann, Faugere, Yannice, Fernández, Vicente, Fleming, Andrew, Garcia-Hermosa, M. Isabel, Sotillo, Marcos García, Garric, Gille, Gasparin, Florent, Giordan, Cedric, Gehlen, Marion, Gregoire, Marilaure L., Guinehut, Stephanie, Hamon, Mathieu, Harris, Chri, Hernandez, Fabrice, Hinkler, Jørgen B., Hoyer, Jacob, Karvonen, Juha, Kay, Susan, King, Robert, Lavergne, Thoma, Lemieux-Dudon, Benedicte, Lima, Leonardo, Mao, Chongyuan, Martin, Matthew J., Masina, Simona, Melet, Angelique, Buongiorno Nardelli, Bruno, Nolan, Glenn, Pascual, Ananda, Pistoia, Jenny, Palazov, Atana, Piolle, Jean Francoi, Pujol, Marie Isabelle, Pequignet, Anne Christine, Peneva, Elisaveta, Pérez Gómez, Begoña, Petit de la Villeon, Loic, Pinardi, Nadia, Pisano, Andrea, Pouliquen, Sylvie, Reid, Rebecca, Remy, Elisabeth, Santoleri, Rosalia, Siddorn, John, She, Jun, Staneva, Joanna, Stoffelen, Ad, Tonani, Marina, Vandenbulcke, Luc, von Schuckmann, Karina, Volpe, Gianluca, Wettre, Cecilie, Zacharioudaki, Anna, Laboratoire d'océanographie de Villefranche (LOV), Institut national des sciences de l'Univers (INSU - CNRS)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS)-Institut de la Mer de Villefranche (IMEV), and Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS)

Subjects
0106 biological sciences, observing systems, Service (systems architecture), services, lcsh:QH1-199.5, 010504 meteorology & atmospheric sciences, Data products, Computer science, satellite, Ocean Engineering, lcsh:General. Including nature conservation, geographical distribution, Aquatic Science, Oceanography, 01 natural sciences, Data assimilation, 14. Life underwater, lcsh:Science, Downstream (networking), data assimilation, 0105 earth and related environmental sciences, Water Science and Technology, Copernicus, Global and Planetary Change, 010604 marine biology & hydrobiology, Perspective (graphical), in situ, ocean, observing system, Marine Sciences, Thematic map, [SDE]Environmental Sciences, Systems engineering, lcsh:Q, Satellite
Abstract

The Copernicus Marine Environment Monitoring Service (CMEMS) provides regular and systematic reference information on the physical and biogeochemical ocean and sea-ice state for the global ocean and the European regional seas. CMEMS serves a wide range of users (more than 15,000 users are now registered to the service) and applications. Observations are a fundamental pillar of the CMEMS value-added chain that goes from observation to information and users. Observations are used by CMEMS Thematic Assembly Centres (TACs) to derive high-level data products and by CMEMS Monitoring and Forecasting Centres (MFCs) to validate and constrain their global and regional ocean analysis and forecasting systems. This paper presents an overview of CMEMS, its evolution, and how the value of in situ and satellite observations is increased through the generation of high-level products ready to be used by downstream applications and services. The complementary nature of satellite and in situ observations is highlighted. Long-term perspectives for the development of CMEMS are described and implications for the evolution of the in situ and satellite observing systems are outlined. Results from Observing System Evaluations (OSEs) and Observing System Simulation Experiments (OSSEs) illustrate the high dependencies of CMEMS systems on observations. Finally future CMEMS requirements for both satellite and in situ observations are detailed.

Published
2019
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197. Ultrasonographic and Histological Correlation after Experimental Reconstruction of a Volumetric Muscle Loss Injury with Adipose Tissue.

Author

Leiva-Cepas, Fernando, Benito-Ysamat, Alberto, Jimena, Ignacio, Jimenez-Diaz, Fernando, Gil-Belmonte, Maria Jesus, Ruz-Caracuel, Ignacio, Villalba, Rafael, and Peña-Amaro, Jose

Subjects
*ADIPOSE tissues, *SKELETAL muscle, *MUSCLE injuries, *MUSCLE regeneration, *ULTRASONIC imaging, *MUSCLES, *TOOTH socket
Abstract

Different types of scaffolds are used to reconstruct muscle volume loss injuries. In this experimental study, we correlated ultrasound observations with histological findings in a muscle volume loss injury reconstructed with autologous adipose tissue. The outcome is compared with decellularized and porous matrix implants. Autologous adipose tissue, decellularized matrix, and a porous collagen matrix were implanted in volumetric muscle loss (VML) injuries generated on the anterior tibial muscles of Wistar rats. Sixty days after implantation, ultrasound findings were compared with histological and histomorphometric analysis. The muscles with an autologous adipose tissue implant exhibited an ultrasound pattern that was quite similar to that of the regenerative control muscles. From a histological point of view, the defects had been occupied by newly formed muscle tissue with certain structural abnormalities that would explain the differences between the ultrasound patterns of the normal control muscles and the regenerated ones. While the decellularized muscle matrix implant resulted in fibrosis and an inflammatory response, the porous collagen matrix implant was replaced by regenerative muscle fibers with neurogenic atrophy and fibrosis. In both cases, the ultrasound images reflected echogenic, echotextural, and vascular changes compatible with the histological findings of failed muscle regeneration. The ultrasound analysis confirmed the histological findings observed in the VML injuries reconstructed by autologous adipose tissue implantation. Ultrasound can be a useful tool for evaluating the structure of muscles reconstructed through tissue engineering. [ABSTRACT FROM AUTHOR]

Published
2021
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198. Antigenicity and immune correlate assessment of seven Plasmodium falciparum antigens in a longitudinal infant cohort from northern Ghana.

Author

Kusi, Kwadwo Asamoah, Aguiar, Joao, Kumordjie, Selassie, Aggor, Felix, Bolton, Jessica, Renner, Andrea, Kyei-Baafour, Eric, Puplampu, Naiki, Belmonte, Maria, Dodoo, Daniel, Gyan, Ben Adu, Ofori, Michael Fokuo, Oduro, Abraham Rex, Atuguba, Frank, Koram, Kwadwo Ansah, Adams, Nehkonti, Letizia, Andrew, Villasante, Eileen, and Sedegah, Martha

Abstract

The current global malaria control and elimination agenda requires development of additional effective disease intervention tools. Discovery and characterization of relevant parasite antigens is important for the development of new diagnostics and transmission monitoring tools and for subunit vaccine development. This study assessed the natural antibody response profile of seven novel Plasmodium falciparum pre-erythrocytic antigens and their potential association with protection against clinical malaria. Antigen-specific antibody levels in plasma collected at six time points from a longitudinal cohort of one-to-five year old children resident in a seasonal malaria transmission area of northern Ghana were assessed by ELISA. Antibody levels were compared between parasite-positive and parasite-negative individuals and the association of antibody levels with malaria risk assessed using a regression model. Plasma antibody levels against five of the seven antigens were significantly higher in parasite-positive children compared to parasite-negative children, especially during low transmission periods. None of the antigen-specific antibodies showed an association with protection against clinical malaria. The study identified five of the seven antigens as markers of exposure to malaria, and these will have relevance for the development of disease diagnostic and monitoring tools. The vaccine potential of these antigens requires further assessment. [ABSTRACT FROM AUTHOR]

Published
2019
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199. Human responses to the DNA prime/chimpanzee adenovirus (ChAd63) boost vaccine identify CSP, AMA1 and TRAP MHC Class I-restricted epitopes.

Author

Ganeshan H, Huang J, Belmonte M, Belmonte A, Inoue S, Velasco R, Maiolatesi S, Limbach K, Patterson N, Sklar MJ, Soisson L, Epstein JE, Edgel KA, Peters B, Hollingdale MR, Villasante E, Duplessis CA, and Sedegah M

Subjects
Humans, Vaccines, DNA immunology, Plasmodium falciparum immunology, Histocompatibility Antigens Class I immunology, Epitopes immunology, Female, Adult, Malaria, Falciparum prevention & control, Malaria, Falciparum immunology, Adenoviruses, Simian immunology, Adenoviruses, Simian genetics, Male, Adenoviridae immunology, Adenoviridae genetics, Interferon-gamma immunology, Interferon-gamma metabolism, Malaria Vaccines immunology, Protozoan Proteins immunology, Protozoan Proteins genetics, Membrane Proteins immunology, Membrane Proteins genetics, Antigens, Protozoan immunology
Abstract

Background: A three-antigen DNA-prime/chimpanzee adenovirus 63 (ChAd63) boost vaccine containing pre-erythrocytic Plasmodium falciparum (Pf) circumsporozoite protein (CSP), Pf apical membrane antigen-1 (AMA1) and malaria multiple epitopes (ME) fused to Pf thrombospondin-related adhesion protein (ME-TRAP) elicited higher vaccine efficacy (VE) in an open label, randomized Phase 1 trial against controlled human malaria infection (CHMI) than the two-antigen vaccine DNA/Human Adenovirus 5 (HuAd5) containing CSP and AMA1. The objective of this follow-up study was to determine whether responses to CSP, AMA1 or TRAP MHC Class I-restricted epitopes were associated with VE., Methodology: Protected (n = 6) and non-protected participants (n = 26) were screened in FluoroSpot interferon gamma (IFN-γ) and Granzyme B (GzB) assays using antigen-specific 15mer peptide subpools spanning CSP (n = 9 subpools), AMA1 (n = 12 subpools), and TRAP (n = 11 subpools). Individual antigen-specific 15mers in the subpools with strong responses were then deconvoluted, evaluated for activities, and MHC Class I-restricted epitopes within the active 15mers were predicted using NetMHCpan algorithms. The predicted epitopes were synthesized and evaluated in the FluoroSpot IFN-γ and GzB assays., Results: Protected and some non-protected participants had similar responses to individual antigen-specific peptide subpools, which did not distinguish only protected participants. However, deconvoluted antigen-specific positive subpools with high magnitudes of responses revealed individual 15mer peptides containing specific and/or predicted MHC Class I (HLA) epitopes. Responses to epitopes were either IFN-γ-only, IFN-γ and GzB, or GzB-only. Due to limitation of cells, most of the analysis concentrated on the identification of protection associated AMA1 epitopes, since most of the predominant pool specific responses were generated against AMA1 15mer subpools. Furthermore, we previously identified protection associated HLA class I-restricted epitopes in a previous gene-based vaccine trial. Seven predicted minimal epitopes in AMA1 were synthesized and upon testing, five recalled responses from protected participants confirming their possible contribution and association with protection, and two recalled responses from non-protected participants. Two protection-associated epitopes were promiscuous and may have also contributed to protection by recognition of different HLA alleles. In addition, strongly positive antigen-specific 15mers identified within active antigen-specific subpools contained 39 predicted but not tested epitopes were identified in CSP, AMA1 and TRAP. Finally, some non-protected individuals recognized HLA-matched protection-associated minimal epitopes and we discuss possible reasons. Other factors such as HLA allele fine specificity or interaction between other HLA alleles in same individual may also influence protective efficacy., Conclusions: This integrated approach using immunoassays and bioinformatics identified and confirmed AMA1-MHC Class I-restricted epitopes and a list of predicted additional epitopes which could be evaluated in future studies to assess possible association with protection against CHMI in the Phase 1 trial participants. The results suggest that identification of protection-associated epitopes within malaria antigens is feasible and can help design potent next generation multi-antigen, multi-epitope malaria vaccines for a genetically diverse population and to develop robust assays to measure protective cellular immunity against pre-erythrocytic stages of malaria. This approach can be used to develop vaccines for other novel emerging infectious disease pathogens., Competing Interests: The authors have declared that no competing interests exist., (Copyright: This is an open access article, free of all copyright, and may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose. The work is made available under the Creative Commons CC0 public domain dedication.)

Published
2025
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200. A randomized clinical trial of the impact of melatonin on influenza vaccine: Outcomes from the melatonin and vaccine response immunity and chronobiology study (MAVRICS).

Author

Lee RU, Watson NL, Glickman GL, White L, Isidean SD, Porter CK, Hollis-Perry M, Walther SR, Maiolatesi S, Sedegah M, Ganeshan H, Huang J, Boulifard DA, Ewing D, Sundaram AK, Harrison EM, DeTizio K, Belmonte M, Belmonte A, Inoue S, Easterling A, Cooper ES, and Danko J

Subjects
Humans, Male, Female, Adult, Middle Aged, Influenza, Human prevention & control, Influenza, Human immunology, Interferon-gamma metabolism, Leukocytes, Mononuclear immunology, Cytokines, Granzymes, Young Adult, Immunogenicity, Vaccine, Immunity, Cellular drug effects, Immunity, Humoral drug effects, Melatonin immunology, Melatonin administration & dosage, Influenza Vaccines immunology, Influenza Vaccines administration & dosage, Antibodies, Viral blood, Hemagglutination Inhibition Tests
Abstract

Vaccine immunogenicity is affected by a variety of factors. Melatonin has been reported to affect immune responses to vaccines and infection. This was a randomized open-label trial - in which adults scheduled to receive the influenza vaccine were randomized to 5 mg melatonin or control to evaluate the effect of post-vaccination melatonin on humoral (hemagglutination-inhibition assays, HAI) and cellular (FluoroSpot) vaccine-specific cytokine responses 14-21 days post-vaccination. A total of 108 participants (melatonin treatment group: 53; control group: 55) completed the study. The groups were similar in baseline characteristics, including sleep as measured by the Pittsburgh Sleep Quality Index. Seroconversion rates or geometric mean fold rises (GMFR) in HAI titers did not vary by treatment group. There were also no statistically significant differences between pre- and post-vaccination levels of interferon gamma (IFN-γ) or granzyme B (GzB) by treatment; however, there was a significantly higher fold rise in the double secretor (IFN-γ + GzB) peripheral blood mononuclear cells for influenza vaccine in subjects taking daily melatonin (GMFR 1.7; 95% CI 1.3, 2.3) compared to those who did not (GMFR 0.9; 95% CI 0.7, 1.1) ( p  < .001). Daily melatonin for 14 days post-influenza vaccination significantly increased the cellular co-expression of IFN-γ + GzB; however, there were no other differences in the cellular or humoral responses. Future studies of the potential utility of melatonin for enhancing vaccine response with larger sample sizes may help elucidate candidate mechanisms for these limited effects, including any interactions with the circadian system.

Published
2024
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